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The role of protein denaturation energetics and molecular chaperones in the aggregation and mistargeting of mutants causing primary hyperoxaluria type I.
[primary hyperoxaluria type 1]
Primary
hyperoxaluria
type
I
(
PH
1
)
is
a
conformational
disease
which
result
in
the
loss
of
alanine
:
glyoxylate
aminotransferase
(
AGT
)
function
.
The
study
of
AGT
has
important
implications
for
protein
folding
and
trafficking
because
PH
1
mutants
may
cause
protein
aggregation
and
mitochondrial
mistargeting
.
We
herein
describe
a
multidisciplinary
study
aimed
to
understand
the
molecular
basis
of
protein
aggregation
and
mistargeting
in
PH
1
by
studying
twelve
AGT
variants
.
Expression
studies
in
cell
cultures
reveal
strong
protein
folding
defects
in
PH
1
causing
mutants
leading
to
enhanced
aggregation
,
and
in
two
cases
,
mitochondrial
mistargeting
.
Immunoprecipitation
studies
in
a
cell-free
system
reveal
that
most
mutants
enhance
the
interactions
with
Hsc
70
chaperones
along
their
folding
process
,
while
in
vitro
binding
experiments
show
no
changes
in
the
interaction
of
folded
AGT
dimers
with
the
peroxisomal
receptor
Pex
5
p
.
Thermal
denaturation
studies
by
calorimetry
support
that
PH
1
causing
mutants
often
kinetically
destabilize
the
folded
apo-protein
through
significant
changes
in
the
denaturation
free
energy
barrier
,
whereas
coenzyme
binding
overcomes
this
destabilization
.
Modeling
of
the
mutations
on
a
1
.
9
Ã…
crystal
structure
suggests
that
PH
1
causing
mutants
perturb
locally
the
native
structure
.
Our
work
support
that
a
misbalance
between
denaturation
energetics
and
interactions
with
chaperones
underlie
aggregation
and
mistargeting
in
PH
1
,
suggesting
that
native
state
stabilizers
and
protein
homeostasis
modulators
are
potential
drugs
to
restore
the
complex
and
delicate
balance
of
AGT
protein
homeostasis
in
PH
1
.
Diseases
Validation
Diseases presenting
"the loss of alanine"
symptom
primary hyperoxaluria type 1
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